(ketofol)
Transcript of (ketofol)
Egyptian Journal of Anaesthesia (2011) 27, 145–150
Egyptian Society of Anesthesiologists
Egyptian Journal of Anaesthesia
www.elsevier.com/locate/egjawww.sciencedirect.com
Research Article
Comparative study between propof, ketamine and their
combination (ketofol) as an induction agent
Hesham Aboeldahab *, Rania Samir, Hesham Hosny, Ahmed Omar
Anesthesia, Faculty of Medicine, Kasr El Aini Hospital, Cairo University, Cairo, Egypt
Received 18 March 2011; accepted 30 April 2011
Available online 18 July 2011
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KEYWORDS
Ketamine;
Propofol;
Ketofol;
Bispectral index
Corresponding author. Tel.:
mail address: h_dahab2005@
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Abstract Introduction: Ketofol is a new combination formed by mixing ketamine and propofol.
This mixture was used for procedential sedation. However, little is known about its hypnotic char-
acteristic as an induction agent.
Methods: Sixty patients were allocated into three equal groups (20 patients each) subjected to hernia
repair surgeries under general anesthesia. These patients were anesthetized using propofol (group
P), ketamine (group K) and ketofol (group KP) as induction agents. The time needed for loss of
verbal contact, eyelash reflex and their corresponding BIS values were recorded. Mean arterial
blood pressure and heart rate were measured. Incidence of apnea, postoperative nausea and vom-
iting, awareness and hallucination were noted.
Results: The time needed for loss of verbal contact and eyelash reflex was earlier in group P fol-
lowed by group KP and group K, respectively, the difference was statistically significant. After
induction, MAP decreased in group P, increased in group K while it remained comparable to base-
line in group KP. The difference between groups was statistically significant. After intubation MAP
increased in the three groups, it was comparable between KP and P groups but remained signifi-
cantly higher in K group. After induction, HR decreased in P group, increased in K group while
it remained comparable to baseline in KP group. The difference between groups was statistically
significant. After intubation HR increased in the three groups, it was significantly higher in group
K in comparison to groups P and KP, and as regards KP group HR was significantly higher than P
group. Afterwards, HR decreased in the three groups and remained stable and comparable for the
7494909.
om (H. Aboeldahab).
Anesthesiologists. Production
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146 H. Aboeldahab et al.
rest of the surgical time. The Bispectral index readings of ketofol group showed intermediate values
between the other two groups.
Conclusion: Ketofol is a safe, effective alternative induction agent that lacks many side effects of its
two components.
ª 2011 Egyptian Society of Anesthesiologists. Production and hosting by Elsevier B.V. All rights reserved.
1. Introduction
Ketamine is an intravenous anesthetic developed in 1960s from
its precursor phencyclidine and its mode of action is throughcausing dissociative anesthesia [1]. Several advantages havebeen attributed to ketamine starting from its amnesic and anal-
gesic effects, maintenance of muscle tone, protecting airway re-flexes and spontaneous respiration. However, ketamine hasmany side effects that limited its frequent use as an anesthetic.
These side effects include nausea, vomiting, emergence halluci-nations, elevation of blood pressure and heart rate due to itssympathomimetic effects and also it was presumed to increaseintracranial pressure [2,3].
Propofol is a 2,6-diisopropylphenol [4] which was devel-oped in Europe in the 1970s, it was utilized progressively inUSA in the subsequent two decades [4,5]. It produces general
anesthesia by facilitation of inhibitory neurotransmission med-iated by GABA. Its main advantages are its rapid inductionand recovery, antiemetic effects and anticonvulsant effects.
Its main disadvantages lie in its dose dependent hypotensionand respiratory depression [6,7].
It was postulated that combining both drugs will result in amixture which has additive effects so that we can decrease the
dose used from each drug and benefit from advantages regard-ing amnesia, analgesia, hypnosis and hemodynamic stabilityand on the other hand lessen the disadvantages attributed to
either drugs [8]. This mixture was named ketofol and was as-sessed as a sedative agent in several studies mainly as in emer-gency departments with encouraging results [8]. In the present
study, we aimed to assess the value of ketofol, when used as aninduction agent, regarding its hypnotic criteria, both clinicallyand by BIS index readings, hemodynamic parameters, and the
incidence of adverse effects of ketofol compared to its two con-stituents ketamine and propofol.
2. Patients and methods
After approval of the ethical research committee in Kasr ElAini hospital Cairo University and obtaining informed written
consent, 60 adult participants aging 20–50 years old, ASAphysical status I and II, without history of cardiovascular orneurologic disease undergoing hernia repair operations were
enrolled in a randomized prospective comparative study. Nopremedication was given to the patients and no medicationswere allowed within 12 h prior to surgery. Upon arrival at
the operating room, preoxygenation was started for 5 min dur-ing which the standard monitors; electrocardiogram, non-inva-sive blood pressure and pulse oximetry were attached to the
patient. BIS monitor electrodes (Aspect Medical System, Vis-taTM, MA, USA) were placed on the skin of the forehead aftercleansing with alcohol. Thereafter baseline vital parameterswere recorded and five successive readings of BIS at 30 s inter-
vals were taken to obtain baseline value while the patients werefully awake, then patients were randomized into three groups,
20 patients each, group K (ketamine), group P (propofol),group KP (ketofol). Methods of randomisation was by aclosed envelope chosen by the surgeon.
Prior to induction, all patients in the three groups received2 ml of lidocaine intravenously to lessen pain on injection espe-cially in the P and KP groups.
Induction of general anesthesia started as follows:
� Group K received intravenous ketamine in a dose of 2 mg/kg over 20 s, syringe contained 200 mg ketamine HCL
(50 mg/ml) mixed with16 ml normal saline to reach a totalvolume of 20 ml given that each ml contained 10 mg of ket-amine and hence 1 ml ketamine syringe for every 5 kg.
� Group P received intravenous propofol 1% in a dose of2 mg/kg over 20 s, given that each ml contained 10 mg pro-pofol and hence 1 ml propofol syringe for every 5 kg.
� Group KP received intravenous ketofol, prepared in a ratioof 1:1 as follows, 100 mg ketamine (50 mg/ml) diluted withglucose 5% to reach a volume of 10 ml + 100 mg propofol1%, total volume is 20 ml each ml containing 5 mg propo-
fol + 5 mg ketamine, the dose given was 1 ml for every 5 kgsupposed to be equipotent to the dose used of each drugsolely in the other two groups.
After 2 min of the start of induction, all patients received2 ucg/kg fentanyl and 0.5 mg/kg atracurium and were mechan-
ically ventilated with isoflurane 1.5% end tidal in 100% O2
using the following parameters: tidal volume 6–8 ml/kg, respi-ratory rate 10–12 min to achieve end tidal CO2 of 30–
35 MmHg, 3 min later the patients were intubated, and main-tained on 1.5% end tidal isoflurane. Intermittent boluses ofatracurium were given throughout the operation and at theend of the surgery any residual neuromuscular block was re-
versed using neostigmine 0.05 mg/kg and atropine 0.02 mg/kg.The patients were then transferred to the post anesthesia careunit (PACU) and discharged when Alderete score was 10 [9].
3. Data collected
� Time needed for loss of verbal contact.� Time needed for loss of eyelash reflex.� BIS values were recorded at the following interval: at base-
line, 5 s after loss of verbal contact, 5 s after loss of eyelashreflex, 2 min after induction, just before intubation, 1 minafter intubation then every 15 min till end of surgery.
� Hemodynamic parameters (mean blood pressure and heartrate) were recorded before induction (taken as a baselinevalue), 2 min after induction, after intubation, 5 min after
intubation and every 15 min till the end of surgery.� All the patients were asked about recall of events or aware-ness and assessed for hallucinations and euphoria in thePACU.
� Incidence of apnea and postoperative nausea and vomitingwas recorded.
Comparative study between propof, ketamine and their combination (ketofol) as an induction agent 147
4. Statistical analysis
Data are statistically described in terms of mean ± SD, fre-
quencies (number of cases) and percentages as appropriate.Continuous data were analyzed done using two-way ANOVAfor repeated measurements with post hoc Tukey’s honest sig-nificant difference test. Qualitative data were compared using
Chi-squared (v2) test with Yates correction. P-values less than0.05 were considered statistically significant. All data were ana-lyzed using SPSS 15.0 for windows (SPSS Inc., Chicago, IL,
USA).
5. Results
There were no significant differences in demographic data be-tween the three groups as regards patients’ age, sex, height,
body weight and ASA physical status (Table 1).Regarding the time needed for loss of verbal contact and
loss of eyelash reflex, patients in group K showed higher read-
ings which were statistically significant relative to the othertwo groups. Patients in group KP lost the reflexes later thanpatients in group P, and there were a statistically significantdifference between the two groups (Table 2).
Table 3 Mean blood pressure (MAP) in MmHg (data are
expressed as mean ± SD) during the follow-up period.
Group P (n= 20) K (n= 20) KP (n= 20)
Baseline 81.50 ± 4.513 82.95 ± 4.98 80.10 ± 4.40
After induction 76.65 ± 4.42c 88.30 ± 4.04a,c 80.65 ± 4.00b
5.1. Regarding hermodynamic effects between groups
� At baseline mean arterial blood pressure was comparable
between groups.� After induction, MAP decreased in group P, increased ingroup K while it remained comparable to baseline in group
KP. The difference between groups was analyzed and foundto be statistically significant.� After intubation MAP increased in the three groups, it wascomparable between KP and P groups but remained signif-
icantly higher in K group. Afterwards, MAP was compara-ble among the three groups (Table 3).
Table 1 Demographic data (data are expressed as mean ±
standard deviation or ratio).
Group P Group K Group KP
Age (years) 30.3 ± 6.3 31.6 ± 6.9 33.45 ± 7.7
Sex; M/F 17/3 16/4 18/2
Height (cm) 166.9 ± 7.16 164.7 ± 7.1 163.3 ± 7.7
Body weight (kg) 81.8 ± 9.26 83.6 ± 8.6 79.2 ± 9.8
ASA grade I/II 10/10 11/9 12/8
Table 2 Time needed for loss of verbal contact and loss of eyelash
Group P
Time for loss of verbal contact (s) 31.80 ± 1.64
Time for loss of eyelash reflex (s) 36.90 ± 2.07
a Statistically significant relative to the other two groups.b Statistically significant relative to group P.
5.2. Regarding heart rate between groups
� Base line heart rate (HR) was comparable between the threegroups.
� After induction, HR decreased in P group, increased in Kgroup while it remained comparable to baseline in KPgroup. The difference between groups was analyzed and
found to be statistically significant.� After intubation HR increased in the three groups, it wassignificantly higher in group K in comparison to groups Pand KP, and as regards KP group HR was significantly
higher than P group.� Afterwards, HR decreased in the three groups especially ingroup K, and remained stable and comparable for the rest
of the surgical time.
5.3. Regarding BIS value between groups
Regarding BIS value, all groups showed BIS values around 95before induction.
With the start of IV induction, patients in the three groupsshowed progressive loss of consciousness proved by loss of ver-bal and eyelash reflexes. BIS values were significantly different
among the three groups as follows:
� In group P, BIS started to decrease with the initiation of IV
injection to reach readings around 65 five seconds after lossof verbal contact and around 50 five seconds after loss ofeyelash reflex, values continued to decrease to reach
reflex (data are expressed as mean ± SD).
Group K Group KP
46.05 ± 1.93a 37.40 ± 2.50b
54.20 ± 2.82a 45.60 ± 2.41b
After intubation 83.25 ± 4.14 91.50 ± 3.54a,c 83.10 ± 4.09
50 0 80.00 ± 3.86 80.25 ± 2.97 82.15 ± 4.20
200 0 82.70 ± 3.65 81.25 ± 2.35 81.20 ± 3.75
350 0 81.30 ± 2.77 81.60 ± 2.23 82.60 ± 3.11
500 0 81.88 ± 2.47 82.40 ± 2.23 81.00 ± 3.17
650 0 82.11 ± 2.14 84.20 ± 2.44 83.10 ± 5.03
800 0 79.40 ± 1.63 80.85 ± 2.92 80.47 ± 3.65
Extubation 85.66 ± 3.43 85.75 ± 2.67 83.90 ± 3.30
P; K; KP.a Statistically significant relative to the other two groups.b Statistically significant relative to group P.c Statistically significant relative to baseline.
Table 6 Regarding postoperative hallucinations, recall or
awareness, it did not occur in any patient in the three groups.
Group P Group K Group KP
Apnea 2 0 0
Nausea or vomiting 0 2 0
Statistically significant relative to group K.
148 H. Aboeldahab et al.
readings around 45 two minutes after start of induction and
these readings were statistically significant relative to theother two groups.� In group K, BIS remained stable in comparison to baseline
readings, values were around 95 five seconds after loss ofverbal contact, 94 five seconds after loss of eyelash reflexand 94 two minutes after induction.� In group KP, BIS started to decrease with the start of IV
injection to reach readings around 85 five seconds after lossof verbal contact and 75 five seconds after loss of eyelashreflex, values continued to decrease to reach readings
around 70 two minutes after start of induction. And thesereadings were statistically significant relative to group K.
After administration of atracurium, fentanyl and ventila-tion with isoflurane 1.5% for 3 min, all readings drifted downin K and KP group to reach a value of 55 while in P group, it
reached a value of 41 (see Tables 4–6).After intubation, readings slightly increased in the three
groups with no statistical significant differences.Five minutes after start of mechanical ventillation all data
were comparable and remained comparable till extubation.
Table 4 Heart rate (HR) (beat/minute)during during the
follow-up period (data are expressed as mean ± SD).
Group P K Ketofol
Baseline 71.95 ± 5.69 72.85 ± 4.47 74.45 ± 6.03
After induction 67.25 ± 3.98 83.70 ± 6.90a,c 78.05 ± 5.20b
After intubation 74.65 ± 4.56 91.70 ± 8.56a,c 80.30 ± 3.61b,c
500 71.01 ± 4.24 83.80 ± 6.03a,c 76.80 ± 4.03b
2000 69.75 ± 3.07 72.35 ± 4.88 71.15 ± 3.08
3500 70.40 ± 4.21 69.85 ± 4.38 71.05±3.08
5000 70.27 ± 6.11 70.95 ± 2.41 71.35±2.45
6500 68.17 ± 3.71 71.15 ± 1.98 69.75±2.26
8000 73.01 ± 1.85 71.95 ± 2.06 73.15±1.97
Extubation 81.73 ± 3.93c 81.65 ± 2.85c 81.65±2.60c
a Statistically significant relative to the other two groups.b statistically significant relative to group P.c statistically significant relative to baseline.
Table 5 Descriptive statistics and test of significance for the
effect of group on BIS during the follow-up period (data are
expressed as mean ± SD).
Group P K Ketofol
Baseline 95.10 ± 0.71 95.30 ± 1.031 95.10 ± 0.71
5 s after loss of verbal 65.01 ± 1.45a 94.65 ± 0.988 85.40 ± 3.78b
5 s after loss of eyelash 50.01 ± 2.65a 94.35 ± 1.089 75.40 ± 2.50b
2 min after induction 45.45 ± 1.64a 94.56 ± 1.319 70.25 ± 3.02�
Before intubation 41.86 ± 2.64a 55.55 ± 1.905 55.00 ± 1.45
After intubation 47.45 ± 2.46a 58.35 ± 1.461 57.80 ± 1.67
500 48.90 ± 3.17 49.95 ± 3.546 50.60 ± 3.06
2000 49.65 ± 3.10 50.40 ± 4.547 49.65 ± 3.10
3500 51.45 ± 3.50 51.45 ± 3.502 52.85 ± 2.34
5000 51.83 ± 3.82 52.05 ± 3.052 52.05 ± 3.05
6500 53.05 ± 3.99 53.05 ± 2.139 53.85 ± 2.64
8000 55.23 ± 2.68 54.50 ± 1.823 53.84 ± 2.52
Extubation 84.10 ± 4.64 83.85 ± 3.760 85.80 ± 3.23
a Statistically significant relative to the other two groups.b Statistically significant relative to group k.
After stoppage of muscle relaxants and inhalational anes-thetics, all the patients regained consciousness within compa-
rable time among the three groups.
5.4. Regarding postoperative nausea and vomiting
� In group K, 2 patients experienced nausea they were treatedwith ondansterone 4 mg.
� In groups P and KP none of the patients experienced nau-sea or vomiting.� Apnea occurred only in propofol group in 2 patients.
Regarding postoperative hallucination, recall or awareness,they did not ocurr in any patient in the three groups.
6. Discussion
The combined use of ketamine and propofol has been ad-dressed with great success in anesthesiology for many years.To the best of our knowledge very little is known in scientificliterature about the use of ketofol (as a drug in a single syringe)
as an induction agent compared to propofol and ketamine[10,11].
The main finding of our study was that when ketofol mix-
ture was used as an induction agent, it showed an intermediateonset of hypnosis relative to its two constituents, providedhemodynamic stability and lower incidence of complications.
In addition, the BIS readings in ketofol group showed interme-diate values relative to the other two groups when correlated tothe clinical end points of hypnosis.
In the current study, the KP group showed intermediate on-
set of clinical hypnosis proved by the time needed for loss ofverbal response and loss of eyelash reflex. In contrast to ourfinding; Frey and his colleagues [12] randomized 70 elderly pa-
tients to receive either propofol in small boluses or propofol insmall boluses with the addition of ketamine (30 mg) in the firstbolus. They demonstrated that the use of ketofol was associ-
ated with shorter time until sedation when compared to propo-fol. In the current study; we used an equipotent dose ofketamine and propofol which could explain the difference be-
tween our findings and their findings.In the study described herein, the ketofol group showed a
more stable hemodynamics in comparison to the other groups.In line with our results, Arora et al. [13] studied 10 adult pa-
tients (over age 18) for procedural sedation given ketofol in1:1 ratio and proved the hemodynamic stability of this mix-ture. Also Akin et al. [14] who found hemodynamic stability
of ketofol in children undergoing cardiac catheterization. Thisis consistent with the result of HUI. et al. [15] who found im-proved cardiovascular stability when using different mixtures
of propofol and ketamine in comparison to either drugs usedsolely.
Comparative study between propof, ketamine and their combination (ketofol) as an induction agent 149
In the KP group, BIS started to decrease with the start of
IV injection to reach values around 85 with the loss of verbalcontact and 75 with loss of eyelash reflex, values continued todecrease to reach readings around 70 two minutes after start ofinduction which is the time needed for both drugs to reach
their peak effect. BIS values in this group could be explainedby the opposing effects of its both constituents upon EEGactivity and hence the reading of BIS. In a study by Sakai et
al. [16] in 1999 who considered the effect of variable doses ofketamine given as a bolus followed by small dose propofoland ketamine infusion on the endpoints of hypnosis and BIS
index, they found additive interaction between propofol andketamine for achieving the hypnotic endpoints; however, themixture did not depress the BIS values in proportion to its
hypnotic effect and this was attributed to the small concentra-tion of propofol used and/or ineffectiveness of ketamine onBIS.
Just before intubation BIS value decreased in the three
groups due to administration of isoflurane and fentanyl toreach a value around 41 in the P group and 55 in the PKand K groups, this finding is supported by studies done by
Bharti and Devrajan, Guignard and by Glass et al. regardingdecrease in Bispectral index when using inhaled anestheticsand opioids [17–19].
After intubation, a rise in the BIS value was observed in thethree groups, it was significantly higher in the KP and K groupthan in the P group but remained within the normal rangeneeded during general anesthesia. Rise in BIS index usually oc-
curs after intubation which is considered a noxious stimulusbut it may be decreased by the use of inhalational anestheticsand opioids as demonstrated by Nakayama et al. and Ropcke
et al. [20,21].Regarding postoperative complication, apnea was defined
as cessation of respiration for >30 s and occurred in 2 patients
in the propofol group which were statistically insignificant rel-ative to the other two groups. Several studies found differentincidences of apnea while using propofol depending on the
dose used, the rate of administration and the definition of ap-nea. In a study by Akin et al. in 2005, 6 out of 30 patients suf-fered from apnea when receiving propofol with a dose of1.5 mg/kg) [10]. Regarding ketofol, apnea did not occur in
any case which could be explained by the fact that the afore-mentioned potential side effect is dose-dependant, and whenused in combination the doses administered of each can be re-
duced [10].Mortero et al. [22] found that adding low-dose ketamine to
propofol sedation attenuated the propofol-induced hypoventi-
lation and preserved the integrity of airway (laryngeal andpharyngeal) reflexes and ventilatory response to carbondioxide.
Regarding PONV, the antiemetic effects of propofol wereevident in the mixture by reducing the number of patientswho suffered from nausea and vomiting from 2 patients inthe K group into no single patient in the KP group. This goes
with the result of Willman and Andolfatto in 2007 [11] whostudied ketofol (1:1 mixture of ketamine 10 mg/mL and propo-fol 10 mg/mL) administered intravenously to One hundred
fourteen patients for procedural sedation and analgesia for pri-marily orthopedic procedures in emergency department andnone of the patients suffered from vomiting in line with our re-
sults also Singh et al. [23], found no patients in their study suf-fered from nausea and vomiting.
The limitations of our conducted study is the small number
of patients, however our results are encouraging regarding theuse of such combination as a safe induction agent with mini-mal side effects. Also we should search for the optimal combi-nation dosage of the two drugs used in the mixture.
7. Conclusion
Ketofol is a safe, effective alternative induction agent thatlacks many side effects of its two components.
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